Nlrp3T346M突变转基因小鼠呈现昼夜节律同步化异常并影响肝脏炎性损伤

doi:10.16352/j.issn.1001-6325.2026.03.0339

基础医学与临床 ›› 2026, Vol. 46 ›› Issue (3): 339-344.doi: 10.16352/j.issn.1001-6325.2026.03.0339

Nlrp3^T346M突变转基因小鼠呈现昼夜节律同步化异常并影响肝脏炎性损伤

王雨鑫, 杨梅, 陈泉霖, 朱蕾^*

中国医学科学院北京协和医学院基础医学研究所药理系,北京 100005

收稿日期:2025-11-14 修回日期:2025-12-24 出版日期:2026-03-05 发布日期:2026-02-25
通讯作者: ^*leizhu2004@126.com
基金资助:
中国医学科学院医学与健康科技创新工程项目(2021-I2M-1-005,2025-I2M-KJ-009);中央高水平医院临床科研业务费(2022-PUMCH-C-025)

Nlrp3^T346M mutant transgenic mice present abnormal circadian entrainment and affect liver inflammatory injury

WANG Yuxin, YANG Mei, CHEN Quanlin, ZHU Lei^*

Department of Pharmacology, Institute of Basic Medical Sciences, Chinese Academy of Medical Sciences & Peking Union Medical College, Beijing 100005, China

Received:2025-11-14 Revised:2025-12-24 Online:2026-03-05 Published:2026-02-25
Contact: ^*leizhu2004@126.com

摘要/Abstract

摘要： 目的基于Nlrp3^T346M突变转基因小鼠,从转录组层面探究NLRP3突变导致其持续活化进而引起肝脏损伤的潜在机制。方法取Nlrp3^T346M小鼠和同窝野生型(WT)小鼠的肝脏组织进行转录组测序,分析两组基因表达差异,对差异表达基因(DEGs)进行GO及KEGG富集分析,RT-qPCR验证相关DEGs的表达情况。结果与WT组相比,Nlrp3^T346M小鼠肝脏中共筛选出258个DEGs,其中上调197个,下调61个。富集分析表明,DEGs主要涉及昼夜节律同步化,以及类固醇、视黄醇、烯烃化合物等的代谢通路。RT-qPCR结果显示,昼夜节律同步化通路中的重要DEGs,即Cacna1h、Camk2b、Gnai1、Mtnr1a和Nos1ap的mRNA变化趋势与转录组结果基本一致。结论 Nlrp3^T346M小鼠肝脏中NLRP3的持续活化可能干扰昼夜节律同步化,进而破坏下游代谢与激素分泌的时序性调控,最终导致肝脏的病理损伤。

关键词: Nlrp3突变, 转基因小鼠, 肝脏, 转录组测序(RNA-seq), 昼夜节律同步化

Abstract: Objective To explore the potential mechanism by which NLRP3 mutation leads to its sustained activation and subsequent liver injury at the transcriptome level with an animal model of Nlrp3^T346M mutant transgenic mice. Methods Liver tissues from Nlrp3^T346M mice and their wild type (WT) littermates were subjected to transcriptome sequencing. Gene expression difference between the two groups was analyzed, followed by GO and KEGG enrichment analyses of the differentially expressed genes (DEGs). RT-qPCR was performed to verify the expression of relevant DEGs. Results Compared with WT group, a total of 258 DEGs were screened in the livers of Nlrp3^T346M mice, of which 197 were up-regulated and 61 were down-regulated. Enrichment analysis showed that the DEGs were mainly involved in circadian entrainment, as well as metabolic pathways of steroids, retinol and olefinic compounds,etc. RT-qPCR results showed mRNA expression trends of key DEGs in the circadian entrainment pathway, namely Cacna1h,Camk2b,Gnai1,Mtnr1a and Nos1ap were consistent with those observed in the transcriptome sequencing. Conclusions Sustained activation of NLRP3 in the liver tissue of Nlrp3^T346M mice may interfere with circadian entrainment, which in turn disrupts temporal regulation of downstream metabolism and hormone secretion, thus leads to liver injury.

Key words: Nlrp3 mutation, transgenic mouse, liver, RNA sequencing(RNA-seq), circadian entrainment

中图分类号:

R967

王雨鑫, 杨梅, 陈泉霖, 朱蕾. Nlrp3^T346M突变转基因小鼠呈现昼夜节律同步化异常并影响肝脏炎性损伤[J]. 基础医学与临床, 2026, 46(3): 339-344.

WANG Yuxin, YANG Mei, CHEN Quanlin, ZHU Lei. Nlrp3^T346M mutant transgenic mice present abnormal circadian entrainment and affect liver inflammatory injury[J]. Basic & Clinical Medicine, 2026, 46(3): 339-344.

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Nlrp3^T346M突变转基因小鼠呈现昼夜节律同步化异常并影响肝脏炎性损伤

Nlrp3^T346M mutant transgenic mice present abnormal circadian entrainment and affect liver inflammatory injury

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Nlrp3T346M突变转基因小鼠呈现昼夜节律同步化异常并影响肝脏炎性损伤

Nlrp3T346M mutant transgenic mice present abnormal circadian entrainment and affect liver inflammatory injury

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Nlrp3^T346M突变转基因小鼠呈现昼夜节律同步化异常并影响肝脏炎性损伤

Nlrp3^T346M mutant transgenic mice present abnormal circadian entrainment and affect liver inflammatory injury